Pharmacokinetics in children with chronic kidney disease · In children, the main causes of chronic...
Transcript of Pharmacokinetics in children with chronic kidney disease · In children, the main causes of chronic...
REVIEW
Pharmacokinetics in children with chronic kidney disease
Anne M. Schijvens1 & Saskia N. de Wildt2,3 & Michiel F. Schreuder1
Received: 28 March 2019 /Revised: 26 June 2019 /Accepted: 2 July 2019# The Author(s) 2019
AbstractIn children, the main causes of chronic kidney disease (CKD) are congenital diseases and glomerular disorders. CKD isassociated with multiple physiological changes and may therefore influence various pharmacokinetic (PK) parameters. Awell-known consequence of CKD on pharmacokinetics is a reduction in renal clearance due to a decrease in the glomerular filtrationrate. The impact of renal impairment on pharmacokinetics is, however, not limited to a decreased elimination of drugs excreted bythe kidney. In fact, renal dysfunction may lead to modifications in absorption, distribution, transport, and metabolism as well.Currently, insufficient evidence is available to guide dosing decisions on many commonly used drugs. Moreover, the impact ofmaturation on drug disposition and action should be taken into account when selecting and dosing drugs in the pediatricpopulation. Clinicians should take PK changes into consideration when selecting and dosing drugs in pediatric CKD patientsin order to avoid toxicity and increase efficiency of drugs in this population. The aim of this review is to summarize known PKchanges in relation to CKD and to extrapolate available knowledge to the pediatric CKD population to provide guidance forclinical practice.
Keywords Pharmacokinetics . CKD . Absorption . Distribution .Metabolism . Excretion . Children
Introduction
Chronic kidney disease (CKD) is a general term for multiple,heterogeneous disorders causing irreversible kidney damage,which is a major public health problem worldwide [1]. Theoverall prevalence in children ranges from 55 to 75 per million[2, 3]. The causes of CKD in children are very different fromadults. In fact, in adults, diabetic nephropathy and hypertensionare the main causes of CKD, whereas CKD in children is oftencaused by congenital diseases and glomerular disorders [2, 3].
The kidneys play an important role in handling of drugs,most importantly in excretion. Awell-known consequence ofCKD on pharmacokinetics (PK) is a reduction in renal
clearance due to a decrease in the glomerular filtration rate(GFR). The impact of renal impairment on the PK of drugsis, however, not limited to a decreased elimination of drugsexcreted by the kidneys. PK describes the individual steps thatdetermine drug disposition in the body, namely absorptionfrom an extravascular site of administration, distribution tovarious tissues, and elimination from the body based on me-tabolism and excretion (Fig. 1). In fact, CKD is associatedwith multiple physiological changes and may therefore influ-ence extrarenal PK processes, which may increase the risk oftoxicity [4–6]. Consequently, patients with impaired kidneyfunction are more at risk of altered drug exposure or toxiceffects than individuals with normal kidney function [7].
Drug dosage adjustment guidelines, based on the assump-tion that systemic clearance primarily reflects renal clearanceand is proportional to kidney function, are commonly used.However, response to drug therapy is often less predictable,which is illustrated by the fact that the frequency of adversedrug reactions and other medication-related problems ishigher in patients with kidney disease than in those with nor-mal kidney function [8, 9]. Despite numerous publishedguidelines regarding drug dosing for patients with reducedkidney function, there is insufficient evidence to guide deci-sions on many commonly used drugs [10]. Moreover, theimpact of maturation on drug disposition and action should
* Anne M. [email protected]
1 Radboud Institute for Molecular Life Sciences, Department ofPediatric Nephrology, Radboud University Medical Center, AmaliaChildren’s Hospital, P.O. Box 9101, 6500HB Nijmegen, The Netherlands
2 Department of Pharmacology and Toxicology, Radboud UniversityMedical Center, Nijmegen, The Netherlands
3 Intensive Care and Department of Pediatric Surgery, Erasmus MCSophia Children’s Hospital, Rotterdam, The Netherlands
https://doi.org/10.1007/s00467-019-04304-9Pediatric Nephrology (2020) 35:1153–1172
/Published online: 2 August 2019
be taken into account when dosing drugs in children.Evidence on the impact of growth and development on ab-sorption, distribution, metabolism, and excretion (ADME) ofdrugs has increased significantly over the years [11].However, the exact interplay between age and disease onPK, pharmacodynamics (PD), and dose requirements remainspoorly understood [11, 12]. Furthermore, the majority ofdrugs prescribed in children are off-label [13, 14], whichlimits the evidence on drug dosing in pediatric CKD patientseven further. Clinicians should take PK changes into consid-eration when selecting and dosing drugs in children with CKDin order to avoid toxicity and to increase efficiency of drugs inthis population. Unfortunately, very little information is avail-able on PK changes in pediatric CKD patients. Therefore, datafrom animal studies, non-CKD children, and clinical studiesin adult CKD patients are used to get an appreciation of thepossible impact of these conditions on the PK in pediatricpatients. The aim of this review is to summarize known PKchanges in relation to CKD with respect to ADME and ex-trapolate available data to the pediatric CKD population toprovide knowledge for clinicians prescribing drugs in thisvulnerable population.
Absorption
Absorption describes the extent to which an intact drug isabsorbed after oral administration from the gut lumen intothe portal circulation. Several factors are known to have animpact on absorption, such as dissolution of the drug, thegastric emptying rate, gastric pH, intestinal motility, drug in-teractions, and passage through the gut wall [15]. Some ofthese factors may vary with growth and development.Ultimately, this may result in changes in the drug absorptivecapacity at different ages in the individual pediatric patient[11]. Maturational changes in the gastrointestinal tract werereviewed by Neal-Kluever et al. [16] and Mooij et al. [17].
The absorption and bioavailability of drugs are highly variablein patients with CKD, in whom several pathophysiologicalchanges in the gastrointestinal tract have been identified thatmay impact drug absorption [4]. Thus far, only little researchhas been conducted to investigate the influence of CKD ondrug absorption in children.
Gastric emptying
Impact of age in non CKD children
Bonner et al. investigated the impact of age and other covariateson the rate of gastric emptying by analyzing published data onapproximately 1500 individuals ranging from premature neo-nates to adults. A model-based meta-analysis indicated that ageitself is not a covariate of gastric emptying [18]. Similarly,Billeaud et al. showed that in children between 0 and 1 yearold, gastric emptying did not vary with age [19]. On the con-trary, Anderson et al. reported slow absorption of acetamino-phen in neonates, with a significant increase in the first days oflife, suggesting fast maturation of gastric emptying in early life[20]. Furthermore, gastric emptying appears to be slower inpreterm neonates compared to term neonates [21].
Adult CKD patients
Patients with CKD may suffer from delayed gastric emptyingfor which several patient characteristics and external factorscan be identified, including peritonitis, peritoneal dialysis, andpharmacotherapy (e.g., aluminum containing antacids, opi-oids) [6, 22]. Results on gastric emptying in adult CKD pa-tients are conflicting, ranging from no obvious impairment toa significant delay in over 30% of the population [23–25].Ultimately, decreased gastric emptying in CKD patients af-fects the time to reach the maximum drug concentrations(Tmax) and peak plasma drug concentration (Cmax) but isnot expected to have an impact on bioavailability [26, 27].
Fig. 1 Overview ofpharmacokinetic processes.ADME absorption, distribution,metabolism, and excretion
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Pediatric CKD patients
Ravelli et al. investigated gastrointestinal function in 12 pedi-atric CKD patients and found both delayed (n = 5) as well asaccelerated (n = 2) gastric emptying [28]. Furthermore, Ruleyet al. showed that gastroesophageal reflux, as a manifestationof gastrointestinal dysmotility, was present in 73% of the pe-diatric CKD patients [29].
Gastric pH
Impact of age in non CKD children
Changes in the gastric pH may influence the bioavailability ofmany drugs. In children, gastric pH is neutral at birth due tofetal ingestion of alkaline amniotic fluid [30]. In the first fewhours after birth, after amnion fluids are removed from thestomach, a rapid decrease in pH is noticed, most likely ex-plained by gastric secretion [30]. Generally, as reviewed byMooij et al., mean gastric pH remains around 2 or 3 in childrenof all ages [17]. Gastric pH rises after feeding; however, as pHrapidly decreases again and most children receive intermittentfeeding, the effect on absorption of acid-labile drugs is limited[31]. On the contrary, one may hypothesize that in childrenwith very frequent or continuous milk-based feeding regi-mens, acid-labile drugs may be absorbed more efficientlydue to a persistent higher gastric pH.
Adult CKD patients
CKD patients often have an increased gastric pH, which mayhave several causes. For instance, patients with renal dysfunc-tion have increased blood urea nitrogen. Excess salivary ureais converted to ammonia by gastric urease enzymes, resultingin increased gastric pH [32, 33]. Furthermore, patients areoften treated with antacids, H2-receptor antagonists, orproton-pump inhibitors that alter gastric pH [34]. Theresulting increase in gastric pH may affect the ionization anddissolution of drugs that are soluble in acidic environments,like furosemide or iron therapy, and reduce their bioavailabil-ity by approximately 20% and 50%, respectively [35, 36].
Pediatric CKD patients
Currently, studies on gastric pH in children with CKD arelimited. However, feeding problems, anorexia, and recurrentvomiting are prevalent problems in pediatric CKD patients[37, 38]. Ravelli et al. investigated the percentage of timespent with an intraesophageal pH below 4 and found signifi-cantly higher mean values in pediatric CKD patients com-pared to age-matched controls. Concomitant drug use was,unfortunately, not reported in these patients [28].
Formation of insoluble salts or metal ion chelates
Some of the drugs administered in patients with CKD mayalter the absorption of other drugs. The ingestion of cation-containing antacids (e.g., sevelamer hydrochloride, lanthanumcarbonate) and minerals (e.g., calcium, magnesium) may re-duce drug absorption because of chelation with co-administered medications, resulting in the formation of insol-uble salts or metal ion chelates [26, 39]. For example, bio-availability of oral ciprofloxacin was significantly decreasedwhen co-administered with sevelamer hydrochloride or calci-um acetate by 48% and 51%, respectively, due to formation ofchelate complexes [39, 40].
Intestinal transport and metabolism
After ingestion, the drug reaches the lumen of the gut, where itmay either diffuse passively or be actively transported by uptaketransporters across the apical membrane into the enterocyte.Once inside the enterocyte, drugs can be actively excreted bytransporters or metabolized by intestinal enzymes [41]. The mostimportant drug metabolizing enzyme family is the cytochromeP450 (CYP) family, with the CYP3A4 isoenzyme as the mostprevalent drug-metabolizing enzyme. The CYP3A subfamily ispresent in the intestine, more specifically in the villi, in abun-dance and contributes to the first-pass metabolism of severalCYP3A4 substrates such as midazolam, cyclosporine, and tacro-limus [42–45]. In addition to the intestine, other organs, includingthe liver, contain a diversity of drug metabolizing enzymes(DMEs) as well [43, 44]. More detailed information regardingDMEs is given in the metabolism section of this review.
Drug transporters are transmembrane proteins facilitatingthe passage of both drugs and other xenobiotics across biolog-ical barriers [46]. Transporters are characterized as either in-flux transporters, which facilitate transport into the cell, orefflux transporters, facilitating the transport out of the cell.The presence of transporters is not limited to the gut [47]. Infact, multiple uptake and efflux transporters are expressed inthe membranes of the intestines, liver and kidneys (for reviewson these transporters, see [48, 49]). An example of an impor-tant drug efflux transporter in the gastrointestinal tract andhepatobiliary system is P-glycoprotein (P-gp). P-gp is anadenosine triphosphate (ATP)-dependent efflux pumpexpressed on the apical membrane of tissues, which are oftenexposed to high concentrations of xenobiotics. The functionof P-gp is to protect the body against toxic compounds bytransporting those out of the cell and the body via the intestinallumen, bile, or urine [50, 51]. Conversely, organic anion-transporting polypeptides (OATP) are a group of uptake trans-porters expressed on the basolateral surface of membraneswith a similar tissue distribution to P-gp [46]. OATP mediatethe transport of mainly organic anions across the cell mem-brane into the cell.
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Impact of age in non CKD children
In general, little is known about transporter gene expression inchildren. Furthermore, evidence on the ontogeny of the differ-ent influx and efflux transporters in children is limited [11, 52].The ontogeny of expression of P-gp was investigated in 59normal duodenal biopsies of children aged 1 month to 17 years.Fakhoury et al. found P-gp mRNA expression levels to behighly variable and unrelated to age [53]. In addition, Mooijet al. observed stable intestinal P-pg mRNA expression fromneonatal to adult age, confirming the aforementioned finding[54]. In contrast, multidrug resistance-associated protein 2(MRP2), another intestinal efflux transporter, showed a differ-ent pattern, with similar mRNA expression levels in neonatesand adults but significantly decreased levels in children aged 1–12 months [54]. Furthermore, intestinal OATP2B1 mRNA ex-pression levels were higher in neonates compared to adults. Inchildren with an age range of 1–12 months, mRNA expressionlevels reached adult values [54]. To our knowledge, no in vivostudies have been conducted to investigate activity of intestinaldrug transporters in pediatric patients. Drug metabolizing activ-ity may change significantly from fetal to adolescent age. Dataregarding the expression of CYP3A enzymes in the gut wall inchildren are contradictory, ranging from an increase with age tothe opposite pattern of a decrease with age. Johnson et al. in-vestigated enterocytic CYP3A expression in duodenal biopsiesin fetuses and children (age range 2 weeks–17 years) and founda significant increase in CYP3A4 expression and activity withage [55]. In contrast, another study showed high CYP3A4mRNA expression levels in the first year of life, followed bya decrease with age [53]. Using a physiological population PKmodeling approach, Brussee et al. simulated intestinal CYP3A4activity per gram of organ to remain relatively constant through-out childhood, indicating that organ growth appears the mostimportant contributing factor to the increase in intrinsic CYP3Aclearance in the gut wall [56]. Using a similar approach, lowCYP3A activity in the gut wall was found in preterm neonates,yielding a low first-pass effect and higher bioavailability in thispatient group compared to adults [57]. The ontogeny of otherintestinal drug-metabolizing enzymes is still largely unknown.
Animal studies
CKD may increase bioavailability of drug substrates due todownregulation of transporters and enzymes in theenterocytes. A decrease in intestinal drug efflux activity maylead to increased bioavailability and increased systemic expo-sure of various drugs, such as calcineurin inhibitors [5].Evidence supporting this phenomenon is mostly based onanimal studies using CKD models [58, 59]. Leblond et al.showed that CKD in rats is associated with a decrease inintestinal CYP1A1 and CYP3A2 activities [60], whereas in-testinal CYP3A function was investigated in several clinical
studies by using phenotyping probes and appeared not to besubstantially altered in patients with end-stage kidney disease(ESKD) [61–63]. Veau et al. found a reduction in intestinaldrug elimination in CKD rats due to a significant decrease inP-gp transport activity without a decrease in protein expres-sion [59]. Moreover, Naud et al. showed a significant reduc-tion in both transport activity as well as protein expression ofintestinal P-gp in CKD rats [58].
Pediatric CKD patients
A frequently observed interaction in pediatric nephrology isthe effect of diarrhea on tacrolimus levels in kidney transplantrecipients. Tacrolimus is extensively metabolized by CYP3A4and is a substrate for P-gp. Oral bioavailability of the drug islow, due to metabolism in the small intestine by CYP3A4 andactive secretion into the gut lumen by P-gp [64]. The concen-tration of CYP3A4 enzymes decreases from the duodenum tothe colon. In case of severe diarrhea, the gastrointestinal transittime is decreased. This could be an explanation for an in-creased oral tacrolimus bioavailability as the drug is shuntedto the colon with lower intestinal metabolism [65].Furthermore, the epithelial cells of the intestine may be dam-aged during the course of diarrhea. This may reduce the en-zymatic activity of CYP3A4 and/or P-gp in the enterocytesand will subsequently lead to increased levels of tacrolimus[66, 67] (Fig. 2). Taken together, CKD-induced reduction inintestinal metabolism and P-gp-mediated drug transport mightresult in increased oral bioavailability of certain drugs.Therefore, a decrease in dose may be necessary for drugs thatare substrates for P-gp and/or CYP3A4 [5, 68].
Bowel wall edema
GI edema has also been identified as a potential cause of altereddrug absorption, particularly in CKD patients with concomitantcirrhosis or congestive heart failure [6, 69]. Bowel wall edemaincreases intestinal permeability and may therefore impair theintestinal barrier function in CKD patients [69].
Distribution
After absorption, drugs distribute to target tissues and sites ofelimination in the systemic circulation. The volume of distri-bution (Vd) represents the parameter relating the concentra-tion of a drug in the plasma to the total amount of the drug inthe body. Several physiologic variables may affect the Vd,including physicochemical properties of the drug (e.g., size,charge, acid dissociation constant, water solubility, lipid solu-bility), plasma protein binding, tissue binding, and total bodywater.With the exception of the physicochemical properties ofthe drug, these variables may be affected in children with
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CKD [4]. Unfortunately, no clinical data are available in pe-diatric kidney transplant patients. Therefore, age-relatedchanges in non CKD children and clinical data in adultCKD patients are summarized below.
Protein binding
Many drugs are extensively bound to plasma proteins, and theVd is highly dependent on the protein binding of the drug.Protein binding limits drug distribution as only the unboundconcentration of the drug is able to cross cellular membranesand distribute outside the vascular space and is therefore
pharmacologically active [41]. The major drug binding pro-teins in plasma are albumin and alpha1-acid glycoprotein(AAG). Acidic drugs are bound to albumin, whereas alkalinedrugs primarily bind to AAG. AAG is an acute phase proteinwith one binding site for alkaline drugs.
Impact of age in non CKD children
Children generally have lower concentrations of the importantbinding proteins, which is most pronounced in newborns andyoung infants [70]. Furthermore, in newborns, fetal albumin(with a reduced binding affinity for weak acids) and
Fig. 2 Impact of CKD anddiarrhea on tacrolimusbioavailability. CKD chronickidney disease, CYP cytochromeP450 enzyme
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endogenous substances, such as bilirubin, are present. Thiscontributes to higher free fractions of highly protein-bounddrugs, due to the capacity of these substances to displace adrug from the albumin binding sites [71]. Clinical implica-tions are especially present for highly protein-bound drugswith a narrow therapeutic index, such as vancomycin [72].
Adult CKD patients
AAG is reported to be increased up to three times in CKDpatients and patients on dialysis as a result of chronicinflammation [34, 73, 74]. In line with this, an increasedplasma binding of alkaline drugs, such as propranolol andcimetidine, has been demonstrated in vitro [75]. In vivoAAG binding, however, generally appears to be unaffect-ed in patients with CKD [34, 75–77]. Plasma proteinbinding of acidic drugs, such as penicillins, cephalospo-rins, furosemide, and phenytoin, is often decreasedin vivo in CKD patients [34, 77]. This decrease has beensuggested to be due to proteinuria- or malnutrition-relatedlow plasma albumin, conformational change of the albu-min binding sites due to uremia, or the accumulation ofcompetitive inflammatory factors, protein-bound uremictoxins, and/or drug metabolites competing with the acidicdrugs for protein binding sites [78, 79]. The last factorappears, however, to be most important [80]. A decreasein protein binding leads to an increase in the unboundfraction of the drug. Generally, this has no significantclinical implications as the unbound drug is readily
available for elimination and distribution in tissues, lead-ing to increased clearance and Vd (Fig. 3). The overalleffect is a new steady-state situation in which the concen-tration of unbound drug and therefore pharmacologicaleffect is unaffected [81]. This phenomenon can be illus-trated by the distribution of phenytoin in CKD patients.Phenytoin is highly protein-bound (90%) in healthy andaround 80% in CKD patients [82], but the pharmacolog-ically active, unbound concentration in plasma is unaffect-ed. The decreased total plasma concentration could bemisinterpreted as a need for dose correction; subsequently,the increase in dose may produce toxicity with no in-creased effectiveness [75]. Ideally, free concentrationsshould therefore be monitored for highly protein-bounddrugs with narrow therapeutic indices in CKD patients.
Tissue binding
Vd may also be affected by altered tissue binding, e.g., inpatients with ESKD. The Vd of digoxin can be reduced by50% due to decreased tissue binding [83–85], potentially dueto a reduction in tissue levels of Na/K-ATPase, the majortissue-binding site for digoxin [86]. The reduction in Vdmay result in increased serum concentrations if the loadingdose is not reduced. However, the pharmacological effect ofdigoxin correlates with the amount of drug in the myocardiumand Jusko et al. reported the myocardium-to-serum concentra-tion ratio of digoxin to decrease in parallel with renal clear-ance [84]. Therefore, a decrease in loading dose may not be
Fig. 3 Decreased protein binding in CKD patients
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necessary. Moreover, as toxic effects also rely on the presenceof tissue binding sites, increased serum concentrations maynot lead to toxic effects [87].
Fluid retention
CKD may cause severe changes in body composition.Furthermore, body composition changes with age and mayaffect the physiological spaces into which a drug will distrib-ute [12]. An already physiological large total body water com-partment in a neonate, combined with a higher total bodywater due to CKD, could result in a significantly increasedVd [13]. Excessive fluid retention, manifesting as increasedextracellular fluid such as edema or ascites, is expected toincrease the Vd of hydrophilic drugs. An increase in extracel-lular fluid volume will have the greatest effect on hydrophilicdrugs with low to moderate Vd (i.e., < 0.7 L/kg), such asaminoglycosides and cephalosporins, resulting in lower plas-ma and tissue concentrations [68]. However, as aminoglyco-sides and cephalosporins are largely excreted unchanged inthe urine, a decrease in kidney function also causes aprolonged half-life and will lead to increased drugconcentrations.
Metabolism
Nonrenal clearance includes all routes of drug elimination,including metabolism, except for renal excretion of un-changed drugs. In fact, only a few drugs are excreted un-changed by the kidney. Metabolism is the major mechanismfor elimination of drugs from the body [88]. Drug metabolismis classified as either a phase I or a phase II reaction. Themajorenzymes responsible for phase I metabolism are the CYP en-zymes [89]. The most abundant CYP enzyme, CYP3A, isresponsible for the metabolism of many drugs [90]. The mostimportant groups of DMEs in phase II metabolism are thesuperfamily of uridine 5′-diphospho-glucuronosyltransferases(UDP-glucuronosyltransferases, UGT). For comprehensiveinformation regarding CYP substrates, inhibitors, and in-ducers, see Flockhart table [91].
Hepatic metabolism
CKD may have various effects on the metabolism of drugs.Decreased protein expression, mRNA expression, and/or ac-tivity of several nonrenal clearance pathways have been re-ported in experimental animal models of CKD [92, 93].Decreased functional expression of hepatic DMEs could leadto a reduction in hepatic clearance of relevant substrates. Thusfar, the exact mechanism by which CKD may affect PK ofnonrenally eliminated drugs is not entirely understood.However, the most important hypothesis is direct inhibition
of non renal clearance pathways by accumulated uremictoxins. Due to kidney failure, molecular breakdown products,which are normally eliminated by the kidneys, now accumu-late in the body. These molecular breakdown products includeurea, inflammatory cytokines, and indoxyl sulfate, also knownas uremic toxins [94, 95]. Uremic toxins cause downregula-tion of gene expression mediated by proinflammatory cyto-kines and directly inhibit the activity of CYP enzymes anddrug transporters.
Impact of age in non CKD children
Maturational changes are well known to occur in the DMEsand have a clear impact on drug disposition in children [96].Age-dependent changes are enzyme and organ specific. Forinstance, hepatic CYP3A7 is present at birth and almost dis-appears after infancy [97]. In contrast, CYP3A4 appears in thefirst week of life and reaches 30–40% of adult activity after1 month [97]. CYP3A4 reaches an adult level of activity at theend of childhood, while CYP3A5 activity appears stable, butwith large genetic variation [90, 96]. While the ontogeny ofhepatic phase I metabolism is increasingly known, our knowl-edge on phase II metabolism lags behind [98]. Awell-knownexample of UGT maturational change is the development ofthe potentially lethal gray baby syndrome in neonates receiv-ing chloramphenicol, which is a consequence of accumulationin the body due to immature glucuronidation by UGT2B7 [99,100]. Similarly, neonatal glucuronidation of morphine (aUGT2B7 substrate) is decreased in newborns compared withadolescents [101, 102]. For additional reviews on metabolismincluding ontogeny of DMEs and age-related changes in me-tabolism of drugs, please see [103, 104].
Animal studies
The expression and activity of CYP3A in CKD patients havebeen studied in several experimental models and clinical stud-ies [93, 105]. Leblond et al. showed a significant decrease intotal liver CYP activity (mainly in CYP2C11, CYP3A1, andCYP3A2) secondary to reduced gene expression in rats withCKD [106, 107]. Furthermore, phase II DMEs may also beaffected by CKD. For example, Simard et al. showed a de-crease in N-acetyltransferase (Nat)1 and Nat2 proteins andNat2 activity secondary to a decrease in gene expression inCKD rats causing a decrease in drug acetylation [108].
Adult CKD patients
Yoshida et al. investigated the effect of CKD on the PK ofin vivo model drugs of CYP3A4/5 in humans and found amodest but variable effect [92]. The effect of CKD on theexpression of CYP3A, however, might be a reflection ofchanges in transporter function rather than a change in enzyme
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activity itself. This hypothesis is supported by the fact that thePK of midazolam, a CYP3A substrate neither a P-gp nor anOATP substrate, is not altered in CKD patients [63]. In con-trast, in vivo CYP2B6, CYP2C19, CYP2D6, and CYP2E1decreased in parallel with the degree of CKD [92, 109].Furthermore, changes to CYP1A2, CYP2C9, and CYP2C8due to CKD appear limited [110, 111]. Osborne et al. showeda significant increase in the area under the curve of morphinein CKD patients compared to control subjects, which suggestsreduced UGT2B7 activity, but a role of the OCT1 transportercannot be excluded [112].
Excretion
Biliary excretion
Biliary excretion eliminates substances from the body whenthe secreted drug is not reabsorbed from the intestine(enterohepatic cycle). Little is known about the developmentalchanges in biliary excretion in children [113]. Alterations invarious biliary efflux transporters have been found in experi-mental models of CKD. An increase in the expression of he-patic efflux transporters, including P-gp, was reportedresulting in an increase in biliary excretion [114]. In contrast,the protein expression of uptake transporter OATP2was foundto be decreased in animal studies, causing a reduction in bil-iary and metabolic clearance [114]. This was confirmedin vivo by Nolin et al. [63].
Renal excretion
Only few drugs are excreted almost entirely unchanged by thekidney, for instance, aminoglycosides and penicillins [115,116]. Renal drug clearance is the net result of three processes:filtration at the glomerulus, active secretion and reabsorptionby the proximal tubule, and passive reabsorption in the kidneytubules. According to the “Intact Nephron Hypothesis,” allsegments of the nephron are equally affected by the develop-ment of any type of renal disease [77, 117]. This suggests that,regardless of the intrarenal pathways of excretion, the loss ofexcretory function in the diseased kidney can be quantified byGFR. However, depending on the cause of renal dysfunction,the normal histology of the glomeruli and the tubules may bedifferentially affected [118].
Glomerular filtration
As blood passes through the glomerulus (± 1000 ml/min in anaverage adult), about 20% of the plasma is filtered into therenal tubule (GFR 120 ml/min). Furthermore, the unbounddrug in plasma water is filtered as well, whereas drugs boundto plasma proteins are not filtered. Glomerular filtration
depends on kidney blood flow, which can decrease when areduced cardiac output or volume depletion is present [5].GFR is often used as an indicator of overall kidney function.
Impact of age in non CKD children
At the transition from fetal to extrauterine life, the glomerularfiltration needs to develop. By 36 weeks of gestation,nephrogenesis is complete [119]. After birth, nephrons areslowly recruited as reviewed by Filler et al. [120]. In termneonates, GFR is just 2–4 ml/min/1.73 m2; it doubles by 1–2 week(s) of age, reaching adult values at approximately 12–24 months of age [121, 122]. Furthermore, GFR continues toincrease after reaching adult values until prepubescent age,resulting in a higher clearance compared to adults [123,124]. The development of GFR is slowed in preterm bornneonates, even though normal values are reached in the end[121]. Maturation of the glomerular filtration and the differentpatterns depending on perinatal circumstances on this matura-tion has a major impact on renal drug clearance.
Adult CKD patients
Endogenous creatinine clearance is frequently used as a mea-sure for GFR. However, a discrepancy may be present be-tween endogenous creatinine clearance and GFR, which ismost pronounced in subjects with low GFR. This is due toan increasing tubular secretion of creatinine with increasingserum creatinine [125, 126]. In that case, creatinine clearanceoverestimates GFR. Moreover, muscle mass is typically de-creased in patients with severe renal dysfunction, leading to areduced production rate [126]. Furthermore, tubular secretionof creatinine can be inhibited by various drugs. Examples ofdrugs that inhibit creatinine secretion include the following:triamterene, spironolactone, amiloride, and trimethoprim[127–129]. In general, the GFR is decreased in CKD patients.According to the Intact Nephron Hypothesis, all segments ofthe nephron are equally affected by the development of anytype of renal disease [77, 117]. This suggests that, regardlessof the intrarenal pathways of excretion, the loss of excretoryfunction in the diseased kidney can be quantified by GFR.However, depending on the cause of renal dysfunction, thenormal histology of the glomeruli and the tubules may bedifferentially affected [118].
In CKD patients, not only the drug itself may accumulate;accumulation of drug metabolites that are primarily excretedby the kidneys may also be an issue [130, 131]. Due to adecrease in GFR, patients will be exposed to prolonged drugeffects or even toxicity if the metabolites are pharmacologi-cally active, especially if a large percentage of the active me-tabolite is excreted unchanged by the kidney under normalcircumstances. A well-known example of this phenomenonis the administration of morphine in CKD patients. Renal
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excretion of morphine itself only accounts for approximately4% of its overall elimination. However, patients with renaldysfunction may show typical signs of morphine intoxicationwhen given standard doses of morphine. Studies have shownthat the major morphine metabolites, which are normally ex-creted by the kidney, extensively accumulate in patients withrenal dysfunction [132, 133]. Thus, despite the fact that thekidneys are only marginally involved in the elimination ofmorphine, patients with CKD can still show signs of morphineintoxication due to accumulation of active metabolites.Moreover, uremic toxins can compete with acidic drugs foractive secretion by the kidney [134].
Active tubular secretion
In the proximal tubule, several transporters are present to fa-cilitate both tubular secretion and tubular reabsorption ofdrugs, exogenous, and endogenous substances. Transportersare localized at the basolateral and apical membranes of theproximal tubular epithelial cells [135]. For some compounds,active secretion is significant and therefore the renal clearanceexceeds the GFR. This is the case with creatinine, but this canalso occur with drugs, such as metformin and amoxicillin[136, 137].
Impact of age in non-CKD children
As reviewed by Brouwer et al., little evidence is available onthe ontogeny of drug transporter expression in the develop-ing human kidney. However, from both animal and humanstudies, one may conclude that renal transporters appear tomature at different rates [113]. Para-aminohippurate clear-ance, a substrate of the organic anion transporter 1 (OAT1),was low at birth, with an increase in the first weeks of neo-natal life, reaching adult levels around 1 year of age[138–140]. Similarly, Momper et al. reanalyzed previouslypublished data on the maximum tubular secretory capacityof PAH (TmPAH) from 119 neonates, infants, and children.TmPAH was low in the immediate postnatal period, in-creased markedly after birth, and reached 50% of the adultvalue at 8 years of age [141]. While PAH clearance mayreflect OAT1 maturation, it cannot be excluded that thesefindings can also be explained by maturation in renalblood flow, as PAH is also a marker of renal bloodflow. Digoxin is excreted by glomerular filtration andextensively secreted in the proximal tubule by P-gp.Pinto et al. investigated age-dependent expression ofrenal P-gp in mice and its correlation with changes inthe clearance rate of digoxin. A significant correlationbetween P-gp expression and digoxin clearance valueswas found [142]. In line with these results, young chil-dren need significantly higher doses of digoxin per ki-logram of body weight than adults. This cannot be
explained by GFR changes alone and may indicatehigher renal P-gp expression in young children than inadults.
Animal studies
Komazawa et al. investigated transport activity of renal trans-porters in CKD rats and showed a decrease in tubular functionin line with a decrease in glomerular filtration. Expressionlevels of organic anion transporter (Oat)1, Oat3, organic cat-ion transporter (Oct)1, and Oct2 were found to be decreased inCKD rats. In contrast, levels of P-gp were significantly in-creased [143]. Similarly, Naud et al. also examined the effectsof CKD on the expression and activity of the major renal drugtransporters in rats. A significant correlation was found be-tween the clearance of creatinine and the protein expressionof transporters. In contrast to Komazawa et al., P-gp wasfound to be significantly reduced [144].
Adult CKD patients
Contrary to the Intact NephronHypothesis, it has been shown that,depending on the underlying cause of CKD, active secretion canincrease relative to glomerular clearance and does not necessarilyshow a decline in parallel with the decline in glomerular filtration[118, 145]. For instance, in patients suffering from glomerulone-phritis, drug clearance may be maintained relative to the reducedGFR by preservation of active tubular secretion [146]. Hsueh et al.reviewed clinical studies regarding the inhibition of OAT1 andOAT3 in CKD patients, and their data suggest that uremic solutescontribute to the decline in renal drug clearance in CKD patientsby inhibition ofOAT1 andOAT3 [147].Onemay hypothesize thatreduction in uptake transporters due to uremic toxins may lead toincreased circulating drug levels in human as well.
Tubular reabsorption
Most of the 120 ml/min of plasma water filtered at the glomer-ulus is reabsorbed during its passage through the renal tubule andin the end only about 1–2 ml/min appears as urine. Reabsorptionof water occurs along the entire nephron, yet, the majority isreabsorbed in the proximal tubule [148]. As plasma water isreabsorbed, a concentration gradient appears between drug inthe tubules and unbound drug in the blood. For the majority ofdrugs and drug metabolites, tubular reabsorption takes place bypassive diffusion. If the drug is able to pass through the mem-branes of the tubular cell, it moves down this concentration gra-dient and is reabsorbed from the tubular fluid back into the blood.Many vital endogenous compounds, including vitamins, electro-lytes, and amino acids, are actively reabsorbed via transporters[148]. Several transporters, such as OAT4, urate transporter 1(URAT1), peptide transporter 2 (PEPT2), organic cation, andcarnitine transporters OCTN1 and OCTN2, reabsorb selected
Pediatr Nephrol (2020) 35:1153–1172 1161
compounds [135]. In line with the maturation of transportersinvolved in tubular secretion, little data are available regardingthe ontogeny of transporters involved in tubular reabsorption, asreviewed by Brouwer et al. [113].
Renal metabolism
As CYP enzyme activity in the human kidney homogenate isabout 14–18% of hepatic enzyme activity [149, 150], renalimpairment could affect renal drug metabolism.
Impact of age in non CKD children
The administration of ifosfamide for the treatment of solid tu-mors in children may illustrate the ontogeny of renal metabo-lism. Ifosfamide is metabolized into the toxic metabolitechloroacetaldehyde [151]. Aleksa et al. investigated the expres-sion of CYP3A expression in pigs, showing low levels in earlylife, followed by a significant increase in both CYP3A expres-sion and ifosfamide metabolism with age followed by a de-crease to adult levels [152]. Subsequently, ontogeny in renalCYP3A enzyme activity may explain why younger children(median age 2.2 years) treated with ifosfamide experience moresevere nephrotoxicity compared to older children [153].
Adult CKD patients
The act ive form of vi tamin D, calc i t r io l (1 ,25-dihydroxycholecalciferol vitamin D3), is taken by patientswith CKD to increase calcium absorption and prevent bonedisease. Metabolic activation of vitamin D (from diet or syn-thesized in the skin) to calcitriol requires hydroxylation of 25-hydroxycholecalciferol at the 1alpha-position in the kidney[154]. Therefore, in patients with CKD, it may be better toadminister vitamin D in the form of calcitriol or 1a-hydroxycholecalciferol [6].
Drug dosing
As summarized in this review, several pharmacokinetic param-eters may be altered in CKD patients. The bioavailability ofcertain drugs may be decreased due to increased gastric pHand formation of insoluble salts, necessitating a dose increase.In contrast, for other drugs, bioavailability may be increaseddue to downregulation of transporters and enzymes inenterocytes, and a lower dose should be administered.Alterations in protein and tissue binding and body compositionmay impact the volume of distribution, requiring an increase ordecrease in dose. Furthermore, CKD may have various effectson drug metabolizing enzymes and transporters. Awell-knowneffect of CKD is a decreased GFR. However, depending on thecause of renal dysfunction, tubular secretion can be affected to a
variable extent. Individual patient and drug characteristicsshould be taken into account when proposing an alternative,individual dosing regimen. In children, developmental changescause variations in absorption, distribution, metabolism, andexcretion over time. All changes should be taken into accountwhen selecting and dosing drugs in children.
Taken together, it is difficult to develop generic drugdosing guidelines for pediatric CKD patients due to alarge variability in PK changes in CKD and maturation-al changes in children. Both sub- and supratherapeuticdosing can occur when the appropriate dose adjustmentsare not made in (pediatric) patients with kidney disease.Subtherapeutic dosing increases the risk of treatmentfailure; supratherapeutic dosing increases the risk of tox-icity. A practical approach to adjusting drug doses inCKD is to assume that renal drug clearance will de-crease in proportion to GFR and that nonrenal clearanceis unchanged, which is also known as the Dettli method[155, 156]. However, this would ignore the role of otherprocesses involved in PK, including the alteration of thefunctional expression of numerous drug metabolizingenzymes and drug transporters and tubular function[4]. In children, PK may be different from adult healthyand CKD patients due to growth and development andthe underlying changes in the processes involved in ab-sorption, distribution, metabolism, and excretion. Linearextrapolation of doses from adults will lead to under- oroverdosing, dependent on the age of the child and therelevant disposition pathways of the drug. In pediatrics,dose adjustments are undertaken to obtain adequate ex-posure and pharmacodynamic effects. Still, to date, forhalf of all drugs, high-quality data are lacking to sup-port the optimal effective and safe drug dose in chil-dren, as reflected by the percentage of drugs being pre-scribed off-label to children [157]. In a project by theDutch Pediatric Formulary, we found that evidence tosupport dosing guidelines in pediatric patients, withCKD, remains especially limited (unpublished data).Consequently, current dosing guidance in pediatric pa-tients with CKD in the Dutch Pediatric Formulary andother dosing guidelines, such as the online PediatricDrug Handbook, is derived from adult data and oftenexcludes young infants and neonates [158, 159].
Nevertheless, although drug-specific data are lackingin this vulnerable population, a few basic principles canbe kept in mind to guide dosing adjustments in childrenwith CKD. The important principles to consider includethe therapeutic index of the drug, the presence of activemetabolites that are eliminated by the kidneys, and theextent of reduction in kidney function. In Table 1, dos-ing advice for pediatric CKD patients is given for a fewdrugs, on the basis of the PK processes affected(ADME). This table includes both commonly prescribed
Pediatr Nephrol (2020) 35:1153–11721162
Table1
Dosingadvice
forpediatricCKDpatientsfor18
differentd
rugs,onthebasisof
thePK
processesaffected
Drug
Vd(L/kg)
PPB
(%)
Modeof
elim
ination
EffectC
KD
T½
N(h)
T½
ESKD
(h)
Requireddosing
GFR
<30
ml/m
in/
1.73
m2
Requireddosing
GFR<15
ml/m
in/
1.73
m2
Ref
Absorption
Propranolol
480–95
Considerablefirstp
asseffect
intheliv
er,alm
ost
completelyexcreted
inthe
urineas
activ
eandinactiv
emetabolites,<5%
unchanged
Increased
bioavailability,
accumulationactiv
emetabolites
2–6
Unchanged
Startwith
smalld
ose,
titrateto
response*
Startwith
smalld
ose,
titrateto
response*
[167,168]
Amitriptylin
e6–36
96Extensive
firstp
ass
metabolism,alm
ost
completelyexcreted
inurine,5%
unchanged.
Increased
bioavailability,
accumulationactiv
emetabolites
9–25
Unchanged
Reducedose
orincrease
dosing
interval*
Reducedose
orincrease
dosing
interval*
[167,168]
Ciprofloxacin
2.5
20–40
10–20%
metabolized,m
ostly
excreted
inurine,40–70%
unchanged
Chelateform
ation
50%
oforaldose
isboundwhengiven
together
with
currently
used
phosphatebinders.
Decreased
renal
clearance.Variable
increase
inelim
inationof
the
drug
viathe
translum
inalroute
across
thebowel
mucosa.
3–5
8Alterdosing
regimen
ofseparatedrugs
50–100%
ofnorm
aldose/in
crease
dose
interval
Alterdosing
regimen
ofseparatedrugs
50%
ofnorm
aldose/in
crease
dose
interval
[158,159,167,
168]
Furosemide
0.07–0.2
91–99
20%
convertedtometabolites.
Mostly
excreted
inthe
urine,largelyunchanged.
Excretedby
tubular
secretion.
Reduced
bioavailability
dueto
increased
gastricpH
.Decreased
protein
binding,increased
Vd.
Impaired
tubular
secretion.
0.5–2
9.7
Normaldose,increased
dosesmay
berequired*
Normaldose,
i ncreaseddoses
may
berequired*
[159,167,168]
Distribution
Oxazepam
0.6–1.6
85–97
Metabolism
byconjugation.
Mostly
excreted
intheurine
asinactiv
emetabolites,
<1%
excreted
unchanged.
Decreased
protein
binding,increased
Vd
3–21
25–90
Normaldose
Startatlowdose,
increase
according
toresponse*
[167,168]
Phenytoin
0.52–1.19
90Extensive
biotransform
ation
intheliv
er,m
ostly
excreted
inthebile.
Decreased
protein
binding
7–42
Unchanged
Normaldose,request
free
phenytoin
concentrations
after
4–5days
Normaldose,request
free
phenytoin
concentrations
after
4–5days
[158,159,167,
168]
Pravastatin
0.5
501.5–2
Unchanged
Startingdose
10mg
Startingdose
10mg
[158,167]
Pediatr Nephrol (2020) 35:1153–1172 1163
Tab
le1
(contin
ued)
Drug
Vd(L/kg)
PPB
(%)
Modeof
elim
ination
EffectC
KD
T½
N(h)
T½
ESKD
(h)
Requireddosing
GFR
<30
ml/m
in/
1.73
m2
Requireddosing
GFR<15
ml/m
in/
1.73
m2
Ref
Biotransformationin
theliv
er,
mostly
excreted
inthe
feces.
Increase
inVd,dueto
fluidretention
Metabolism
Captopril
225–30
40%
hepatic
metabolism,65%
excretionviaurine,
40–50%
unchanged.
Decreased
clearance
2.3
21Startlow,titrateto
response.
75%
ofnorm
aldose
Startlow,titrateto
response.
50%
ofnorm
aldose
[159,167,168]
Repaglin
ide
0.4
>98
HepaticCYP3
A4metabolism
toinactiv
emetabolites,
excretionviabile.
Decreased
clearance
12
Startlow,titrateto
response*
Startlow,titrateto
response*
[167,168]
Reboxetine
26-63L
97HepaticCYP3
A4metabolism
toinactiv
emetabolites,
elim
inationin
urine,10%
unchanged
Decreased
clearance
1326
50%
ofinitialdose,
adjustaccordingto
response
50%
ofinitialdose,
adjustaccordingto
response
[167,168]
Renalmetabolism
Insulin
0.15
5Hepaticandrenalm
etabolism,
1–1.5%
unchanged
excretionin
urine
Decreased
clearance
2–5
13Variable,basedon
glucoselevels.
Variable,basedon
glucoselevels.
[168]
Vitamin
D–
–Renalmetabolism
Noconversion
toactiv
eform
––
Use
activ
eform
Use
activ
eform
[167]
Excretio
n
Benzyl-penicillin
0.5–0.6
60Alm
ostcom
pletelyexcreted
unchangedin
urine.
Decreased
clearance
0.5
1050%,doseinterval12
h25–50%
,doseinterval
12-16h
[167,168]
Aciclovir
0.7
9–33
Predominantly
excreted
inurine,>80%
unchanged
Decreased
clearance
2.9
19.5
100%
dose,dose
interval24
h50%
dose,dose
interval24
h[158,159,167,
168]
Fluconazole
0.65–0.7
11–12
>90%
excreted
intheurine,
80%
unchanged.
Decreased
clearance
3098
50%
ofnorm
aldose,
dose
interval24
h50%
ofnorm
aldose,
dose
interval
24-48h
[158,159,167,
168]
Morphine
3–5
20–35
Hepaticconjugation,10%
excreted
unchangedinurine
Decreased
clearance.
Accum
ulationof
activ
emetabolites
(morphine-6--
glucuronide,
morphine-3--
glucuronide)
2.5
Active
metabolite
3–5
Unchanged
Active
metabolite
50
Smalld
oses,extended
dosing
intervals,
titrateto
response.
75%
ofnorm
aldose.
Considersw
itchto
alternativedrug
(e.g.,
piritram
ide)
Smalld
oses,extended
dosing
intervals,
titrateto
response.
50%
ofnorm
aldose.
Considersw
itchto
alternativedrug
(e.g.,piritram
ide)
[158,159,167,
168]
Vancomycin
0.47–1.1
10–50
80–90%
excreted
unchanged
inurine
Decreased
clearance
6120–216
100%
ofnorm
aldose,
increase
dose
interval
to48–72h
100%
ofnorm
aldose,
increase
dose
intervalto
1week
[158,159,167,
168]
Amikacin
0.22–0.29
<20
94–98%
excreted
unchanged
inurine
Decreased
clearance
2–3
17–150
Dosereductionand
increase
dose
interval
basedon
drug
levels*
Dosereductionand
increase
dose
intervalbasedon
drug
levels*
[158,159
167,
168]
Pediatr Nephrol (2020) 35:1153–11721164
drugs and drugs that are illustrative of one of the spe-cific PK processes.
Basic principles of dose adjustments in CKD
Drug exposure relates to the maximum plasma concentrationand/or the area under the concentration time curve (AUC). Ingeneral, supra-therapeutic exposures increase the risk of dose-related adverse drug reactions, and subtherapeutic exposure in-creases the risk of ineffective therapy. As infections are com-mon in patients with CKD, basic knowledge on thepharmacodynamic properties of antibiotics is necessaryto optimize treatment, as was recently reviewed byMomper et al. [160]. For antibiotics, three PK-PD tar-gets describe features of the concentration-time profilethat maximize antibiotic efficacy (Fig. 4):
1. The ratio of maximum free drug plasma concentration tom i n imum i n h i b i t o r y c o n c e n t r a t i o n (M IC )(aminoglycosides)
2. The ratio of AUC to MIC (vancomycin)3. The proportion of time that the plasma concentration ex-
ceeds the MIC (β lactam antibiotics)
For each individual drug, the PK-PD target should betaken into account when prescribing the dosing regimen.Dose adjustments for primarily hepatically metabolizeddrugs should be carefully considered as well, as theirpharmacologically active and/or toxic metabolites canbe excreted by the kidney, e.g., morphine and mycophe-nolate mofetil [161, 162]. The minimum change in kid-ney function that requires a change in dose is not welldefined [5]. In general, dose adjustment is unlikely tobe required when < 30% of the dose is excreted by thekidney [5, 163]. However, in drugs with a small thera-peutic index, this statement should be reconsidered.
Loading dose
Some drugs and clinical situations, for instance antibiotics inpatients with a severe infection, require rapid therapeutic con-centrations. The time to reach steady state is determined by thehalf-life (T1/2), and it takes three to five half-life periods to reachsteady state. Half-life is a PK parameter determined by bothclearance (CL) and Vd (T1/2 = 0.693 ×Vd/CL). When T1/2 isprolonged, the time to reach steady state increases proportion-ally. Hence, for some drugs, a loading dose is necessary todecrease the time needed to reach the plateau drug concentra-tion. The loading dose to achieve a target concentration is de-termined by the Vd (loading dose = target concentration × Vd).However, when CKD coincides with an altered volume of dis-tribution of a drug, the loading dose must be modified [134].T
able1
(contin
ued)
Drug
Vd(L/kg)
PPB
(%)
Modeof
elim
ination
EffectC
KD
T½
N(h)
T½
ESKD
(h)
Requireddosing
GFR
<30
ml/m
in/
1.73
m2
Requireddosing
GFR<15
ml/m
in/
1.73
m2
Ref
Gentamicin
0.3
0–30
90%
excreted
unchangedin
urine
Decreased
clearance
2–3
20Dosereductionbasedon
drug
levels,increase
dose
intervalto48
h*
Dosereductionand
increase
dose
intervalbasedon
drug
levels*
[158,159
167,
168]
Tobram
ycin
0.25
<5
90%
excreted
unchangedin
urine
Decreased
clearance
2–3
5–70
Dosereductionbasedon
drug
levels*
Dosereductionand
increase
dose
intervalbasedon
drug
levels*
[158,159
167,
168]
CKD
chronickidney
disease,ESK
Dend-stagekidney
disease,GFRglom
erular
filtrationrate,h
hours,Nnorm
al,N
Dno
data,P
PBplasmaproteinbinding,
Refreferences,T
½half-life,Vdvolumeof
distributio
n
*Noexactd
oserecommendatio
nsor
contradictorydose
recommendatio
nsareavailablein
theliterature
Pediatr Nephrol (2020) 35:1153–1172 1165
Maintenance dose
The maintenance dose is aimed at maintaining thedesired steady-state drug concentrations. The mainte-nance dose is determined by the drug concentration atsteady state (Css) and the CL of the drug from thebody (maintenance dose = Css × CL). For intermittentdosing, the desired dosing interval should be takeninto account as well. A decrease in drug clearancewith kidney disease necessitates, therefore, a decreasein either maintenance dose, an increase in the dosinginterval, or both [34]. The dosing frequency dependson the toxicity profile of the drug. An importantquestion to consider is whether the effects of the drugrelate to the peak or to average exposure of the drug.A relatively long dosing interval will require a rela-tively high Cmax to maintain an acceptable meandrug concentration or AUC. Therefore, in most in-stances, a reduction in dose rather than an increasein dosing interval is appropriate, with the exceptionof drugs where high peak serum concentrations arebeneficial such as gentamicin and tobramycin.
Research priorities
As stated in the KDIGO guideline on CKD evaluationand management, national and international researchgroups should ensure adequate representation of adultCKD patients in clinical trials to improve the under-standing of PK and PD parameters in this population[164]. Moreover, drug research involving pediatric indi-cations and drug dosing optimization in pediatric clinical
practice is challenging. Limited observational data canbe used to create dosing advice for specific drugs andpatient categories, as we previously demonstrated [165].Furthermore, physiologically based pharmacokinetic(PBPK) modeling can be used to predict the pharmaco-kinetic behavior of drugs in humans using preclinicaldata [166]. For the pediatric (CKD) population, we be-lieve that PK studies and PBPK modeling should be usedto incorporate pediatric developmental physiology anddisease to predict drug exposure in vulnerable patientgroups. Currently, several initiatives are in progress todetermine the population PK of, for instance, antibiotics(NCT03248349, NCT02539407) and antiretroviral drugs(NCT03194165) in the pediatric (non-CKD) population.
Conclusion
CKD is a heterogeneous condition, which is a major publichealth problem worldwide. In patients with CKD, the PK ofseveral drugs can be significantly altered. For pediatric CKDpatients, the impact of maturation on drug disposition and actionshould be taken into account aswell. As shown in this review, theeffects may be variable and are not limited to renal drug clear-ance. In fact, CKD may also have a major influence on drugabsorption, distribution, and drug metabolism in the liver, gut,and kidneys. Inappropriate dose adjustments may lead to sub- orsupratherapeutic concentrations predisposing the patient to eithertherapeutic failure or adverse drug reactions. As general guide-lines in pediatric CKD patients are lacking, prescribing an appro-priate dose requires knowledge on specific PK alterations in thisstudy population. Finally, we believe that all available data
Fig. 4 Concentration-time profileof antibiotics. Peak/MIC: Theratio of maximum free drugplasma concentration to the MIC.AUC/MIC: The ratio of the totalexposure of the drug to the MIC.Time/MIC: The proportion oftime that the plasma concentrationexceeds the MIC. AUC areaunder the concentration timecurve, Cmax maximumconcentration, MIC minimuminhibitory concentration for apathogen, T time
Pediatr Nephrol (2020) 35:1153–11721166
should be used to extrapolate dosing advice in the adult popula-tion to the pediatric CKD population.
Multiple choice questions
1. Which of the following pharmacokinetic processes maybe altered in patients with CKD?
a) Absorptionb) Distributionc) Metabolismd) Eliminatione) All of the above
2. In case of CKD, the dose of a drug should be reduced.
a) Yesb) Noc) Depends on the drug given
3. Where does metabolism take place in the body?
a) Liverb) Kidneysc) Gutd) All of the above
4. Which dose should be adjusted in case of a decreasedGFR?
a) Loading doseb) Maintenance dosec) Both
5. All drug metabolizing enzymes will increase with age
a) Trueb) False
Funding This study was funded by the Dutch Kidney Foundation (grantnumber 15OKG16).
Compliance with ethical standards
Conflict of interest The authors declare that they have no conflict ofinterest.
Open Access This article is distributed under the terms of the CreativeCommons At t r ibut ion 4 .0 In te rna t ional License (h t tp : / /creativecommons.org/licenses/by/4.0/), which permits unrestricted use,distribution, and reproduction in any medium, provided you give appro-priate credit to the original author(s) and the source, provide a link to theCreative Commons license, and indicate if changes were made.
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